Department of Surgery, Emory University School of Medicine, Atlanta, GA, USA.
Emory Winship Cancer Institute, Atlanta, GA, USA.
Nat Commun. 2024 Jun 20;15(1):5280. doi: 10.1038/s41467-024-49475-8.
The regulatory circuits dictating CD8 T cell responsiveness versus exhaustion during anti-tumor immunity are incompletely understood. Here we report that tumor-infiltrating antigen-specific PD-1 TCF-1 CD8 T cells express the immunosuppressive cytokine Fgl2. Conditional deletion of Fgl2 specifically in mouse antigen-specific CD8 T cells prolongs CD8 T cell persistence, suppresses phenotypic and transcriptomic signatures of T cell exhaustion, and improves control of the tumor. In a mouse model of chronic viral infection, PD-1 CD8 T cell-derived Fgl2 also negatively regulates virus-specific T cell responses. In humans, CD8 T cell-derived Fgl2 is associated with poorer survival in patients with melanoma. Mechanistically, the dampened responsiveness of WT Fgl2-expressing CD8 T cells, when compared to Fgl2-deficient CD8 T cells, is underpinned by the cell-intrinsic interaction of Fgl2 with CD8 T cell-expressed FcγRIIB and concomitant caspase 3/7-mediated apoptosis. Our results thus illuminate a cell-autonomous regulatory axis by which PD-1 CD8 T cells both express the receptor and secrete its ligand in order to mediate suppression of anti-tumor and anti-viral immunity.
调控 CD8 T 细胞在抗肿瘤免疫中应答与耗竭的调控回路尚不完全清楚。在这里,我们报告肿瘤浸润的抗原特异性 PD-1 TCF-1 CD8 T 细胞表达免疫抑制细胞因子 Fgl2。在小鼠抗原特异性 CD8 T 细胞中特异性缺失 Fgl2 可延长 CD8 T 细胞的持久性,抑制 T 细胞耗竭的表型和转录组特征,并改善肿瘤控制。在慢性病毒感染的小鼠模型中,PD-1 CD8 T 细胞衍生的 Fgl2 也负调控病毒特异性 T 细胞反应。在人类中,CD8 T 细胞衍生的 Fgl2 与黑色素瘤患者的生存率较差相关。从机制上讲,与 Fgl2 缺陷型 CD8 T 细胞相比,WT Fgl2 表达的 CD8 T 细胞应答能力下降,这是由 Fgl2 与 CD8 T 细胞表达的 FcγRIIB 的细胞内相互作用以及伴随的 caspase 3/7 介导的细胞凋亡所支撑的。因此,我们的研究结果阐明了一个细胞自主调节轴,PD-1 CD8 T 细胞通过该轴既能表达受体又能分泌其配体,从而介导抗肿瘤和抗病毒免疫的抑制。
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